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Distinct roles of GABAB1a- and GABAB1b-containing GABAB receptors in spontaneous and evoked termination of persistent cortical activity

机译:含Gabab1a和GabaB1b的含有含有持续性皮质活动终止的含GabaB1和GabaB1B的含Gabab受体的不同作用

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摘要

During slow-wave sleep, cortical neurons display synchronous fluctuations between periods of persistent activity (UP states') and periods of relative quiescence (DOWN states'). Such UP and DOWN states are also seen in isolated cortical slices. Recently, we reported that both spontaneous and evoked termination of UP states in slices from the rat medial entorhinal cortex (mEC) involves GABAB receptors. Here, in order to dissociate the roles of GABAB1a- and GABAB1b-containing receptors in terminating UP states, we used mEC slices from mice in which either the GABAB1a or the GABAB1b subunit had been genetically ablated. Pharmacological blockade of GABAB receptors using the antagonist CGP55845 prolonged the UP state duration in both wild-type mice and those lacking the GABAB1b subunit, but not in those lacking the GABAB1a subunit. Conversely, electrical stimulation of layer 1 could terminate an ongoing UP state in both wild-type mice and those lacking the GABAB1a subunit, but not in those lacking the GABAB1b subunit. Together with previous reports, indicating a preferential presynaptic location of GABAB1a- and postsynaptic location of GABAB1b-containing receptors, these results suggest that presynaptic GABAB receptors contribute to spontaneous DOWN state transitions, whilst postsynaptic GABAB receptors are essential for the afferent termination of the UP state. Inputs to layer 1 from other brain regions could thus provide a powerful mechanism for synchronizing DOWN state transitions across cortical areas via activation of GABAergic interneurons targeting postsynaptic GABAB receptors.
机译:在慢波睡眠期间,皮质神经元在持续活动(UP状态')之间的同步波动和相对静态(下态')之间的同步波动。在孤立的皮质切片中也可以看到如此脱下的状态。最近,我们报道称,从大鼠内侧梭菌皮质(MEC)的切片中的自发和诱发终止终止涉及纳布夫受体。这里,为了解散含GabaB1A和GabaB1B的受体在终止状态中的作用,我们使用来自小鼠的MEC切片,其中GABAB1A或GABAB1B亚基已遗传烧蚀。使用拮抗剂CGP55845的Gabab受体的药理阻滞延长了野生型小鼠的UP状态持续时间,缺乏GABAB1B亚基的那些,但不是在缺乏GABAB1A亚基的那些中。相反,层1的电刺激可以在野生型小鼠中终止持续的状态,并且缺乏GABAB1A亚基的那些,但不是在缺乏GABAB1B亚基的那些中。连同之前的报道,表示GABAB1a-的优惠突触前位置,并含GABAB1b受体的突触后的位置,这些结果表明,突触前受体GABAB有助于自发DOWN状态转换,而突触后GABAB受体是UP状态的传入终止必不可少。因此,来自其他脑区的层1的输入可以通过靶向突触后纳布纳受体的胃肠杆菌性间核激活来提供一种强大的机制,用于通过激活胃肠杆菌的胃肠杆菌的中间核来同步皮质区域跨皮质区域的转变。

著录项

  • 来源
    《The Journal of Physiology》 |2013年第4期|共9页
  • 作者单位

    Eunice Kennedy Shriver Natl Inst Child Hlth &

    Hum Program Dev Neurobiol NIH Bethesda MD 20892;

    Eunice Kennedy Shriver Natl Inst Child Hlth &

    Hum Program Dev Neurobiol NIH Bethesda MD 20892;

    Univ Basel Inst Physiol Dept Biomed CH-4056 Basel Switzerland;

    Univ Oxford Dept Physiol Anat &

    Genet Oxford OX1 3PT England;

    Eunice Kennedy Shriver Natl Inst Child Hlth &

    Hum Program Dev Neurobiol NIH Bethesda MD 20892;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 人体生理学;
  • 关键词

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